<i>vps25</i>mosaics display non-autonomous cell survival and overgrowth, and autonomous apoptosis

Herz, Hans-Martin; Chen, Zhihong; Scherr, Heather; Lackey, Melinda; Bolduc, Clare; Bergmann, Andreas

doi:10.1242/dev.02356

Cited by 148 publications

(266 citation statements)

References 70 publications

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“…However, as we and others have reported, in imaginal discs mosaic for strong alleles of the neoplastic TSGs scrib, lgl, dlg, avl, and Rab5, homozygous mutant cells are usually lost due to the process of cell competition (Brumby and Richardson 2003;Pagliarini and Xu 2003;Zeitler et al 2004;Uhlirova et al 2005). Tsg101 and vps25 cells survive competition but, like cells mutant for all neoplastic TSGs, fail to differentiate and do not contribute to the adult eye (Moberg et al 2005;Thompson et al 2005;Vaccari and Bilder 2005;Herz et al 2006). Thus, in a genetically mosaic imaginal disc, neoplastic mutant cells do not overgrow to form a tumor that can be easily detected in either larvae or adults.…”

Section: Resultsmentioning

confidence: 70%

“…Three of these-scrib, dlg, and lgl-encode cytoplasmic proteins with various protein-protein interaction domains ( Jacob et al 1987;Woods and Bryant 1991;. Four others-avl, Rab5, tsg101, and vps25-encode components of the endocytic machinery (Lu and Bilder 2005;Moberg et al 2005;Thompson et al 2005;Vaccari and Bilder 2005;Herz et al 2006). The relationship between the cytoplasmic scaffolds and the endocytic regulators, the mechanism of action of these proteins in cell polarity, and in particular how they each act to restrain cell proliferation remains mysterious.…”

Section: T He Imaginal Discs Of the Drosophila Larva Havementioning

confidence: 99%

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A Mosaic Genetic Screen for Drosophila Neoplastic Tumor Suppressor Genes Based on Defective Pupation

et al. 2007

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The Drosophila neoplastic tumor suppressor genes (TSGs) coordinately control cell polarity and proliferation in epithelial and neuronal tissues. While a small group of neoplastic TSG mutations have been isolated and their corresponding genes cloned, the regulatory pathways that normally prevent inappropriate growth remain unclear. Identification of additional neoplastic TSGs may provide insight into this question. We report here the design of an efficient screen for isolating neoplastic TSG mutations utilizing genetically mosaic larvae. This screen is based on a defective pupation phenotype seen when a single pair of imaginal discs is homozygous for a neoplastic TSG mutation, which suggests that continuously proliferating cells can interfere with metamorphosis. Execution of this screen on two chromosome arms led to the identification of mutations in at least seven new neoplastic TSGs. The isolation of additional loci that affect hyperplastic as well as neoplastic growth indicates the utility of this screening strategy for studying epithelial growth control.

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Section: Resultsmentioning

confidence: 70%

Section: T He Imaginal Discs Of the Drosophila Larva Havementioning

confidence: 99%

A Mosaic Genetic Screen for Drosophila Neoplastic Tumor Suppressor Genes Based on Defective Pupation

et al. 2007

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“…Fourth, clones of a different mutant, vps25, which is characterized by strong N activity, cause non-autonomous accumulation of Diap-1 protein. 26 Fifth, clones of cells expressing the active form of N (N intra ) cause non-cell autonomous accumulation of Diap-1 in neighboring cells (Figures 5g, g 0 and g 00 ). This observation demonstrates that N does not directly induce diap1 transcription, but generates another signal that promotes diap1 …”

Section: Resultsmentioning

confidence: 99%

“…The autonomy of GMR-hid suppression was examined with GMR-hid[w -], an insertion on the third chromosome. 26 hs-FLP was used to induce mosaic wing discs. Mosaics were also generated using the MARCM (mosaic analysis with a repressible cell marker) technique, which allows expression of transgenes such as UAS-CiR in mutant clones.…”

Section: H29mentioning

confidence: 99%

Non-cell autonomous control of apoptosis by ligand-independent Hedgehog signaling in Drosophila

et al. 2012

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“…Notch and Janus kinases-signal transducers and activators of transcription (JAK-STAT) signal pathways were associated with proliferation, which can be induced by apoptosis (Moberg et al, 2005;Thompson et al, 2005;Vaccari and Bilder, 2005;Herz et al, 2006). Mutations in ubiquitin-like modifier activating enzyme 1, which catalyzes the activation stage in the ubiquitin conjugation pathway, induce apoptosis directly and tissue growth indirectly.…”

Section: Caspases In Cell Proliferationmentioning

confidence: 99%

A matter of regeneration and repair: caspases as the key molecules

Bolkent¹,

Öztay²,

Oktayoğlu³

et al. 2016

Turk J Biol

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Researchers have been focused on understanding the pathogenesis of human diseases. They have been working to find the roles of caspases in the balance between apoptosis, autophagy, pyroptosis, and necroptosis, and also in the regeneration of damaged tissue. At this point, besides their death-inducing roles, new findings indicate the role of caspases in proliferation for maintaining the viability of cells in response to signals from apoptotic cells. Recently, determining cell fate has also been identified among other functions of caspases. Findings indicate that caspases direct cellular pathways to cell differentiation by suppressing stem cell self-renewal. The common opinion about the related mechanism is that low and transient caspase activation leads to terminal differentiation by affecting the expression of key genes related to differentiation. Moreover, caspases are essential proteases in the regulation and modulation of the repair process. In repair, they have roles in apoptosis, release of inflammatory cytokines and chemokines, promotion of cell migration, and immune cell infiltration. However, paracrine signaling through caspase activation leads to cell proliferation after cancer therapy and causes tumor relapse, which complicates the current therapy. In this scope, we have reviewed the main mechanisms of pathological, regenerative, and restorative effects of caspases.

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vps25mosaics display non-autonomous cell survival and overgrowth, and autonomous apoptosis

Cited by 148 publications

References 70 publications

A Mosaic Genetic Screen for Drosophila Neoplastic Tumor Suppressor Genes Based on Defective Pupation

A Mosaic Genetic Screen for Drosophila Neoplastic Tumor Suppressor Genes Based on Defective Pupation

Non-cell autonomous control of apoptosis by ligand-independent Hedgehog signaling in Drosophila

A matter of regeneration and repair: caspases as the key molecules

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